Abstract

Several processes are regulated by interfacial catalysis on the membrane surfaces. Thus phospholipase A2 (PLA2) are interesting not only as prototypes for interfacial catalysis in general, but also because they mobilize precursors for the biosynthesis of eicosanoids and platelet activating factor, which ultimately control a wide range of secretory and inflammatory processes. The long range objective of our studies on interfacial catalysis is to gain detailed kinetic, biophysical, and molecular knowledge about PLA2 at the interface. An understanding of the mechanism would also help in the design, assay and characterization of specific inhibitors, which could be useful in establishing and controlling the biological functions of PLA2. During the next five years we plan to use the kinetic and equilibrium methods developed recently in our laboratory for pig PLA2 (type I) to achieve the following objectives: (a) to obtain the equilibrium and kinetic parameters for other PLA2, such as the cloned type II enzyme from synovial fluid, the type III PLA2 from bee venom, and the arachidonate-specific 89 KD enzyme from the cytoplasm of a human cell line; (b) to characterize the amino acid residues exposed to the aqueous phase on the enzyme bound to the interface; (c) to spectroscopically characterize the E, E*, and E*L forms of PLA2; (d) to establish if the catalytic or the product release step is rate-limiting during the catalytic turnover; (e) to investigate the kinetics of hydrolysis of short chain substrates under the conditions where they are dispersed as solitary monomers, so as to obtain insights into the possibility of the formation of a solitary ES complex; (f) to characterize the kinetics of hydrolysis of long chain phospholipids codispersed with bile salts to examine if on small aggregates the rate of hydrolysis is limited by the rate of replenishment of the substrate. By integrating the information obtained from such studies, we hope to obtain a general and complete kinetic description of interfacial catalysis by PLA2 from several sources. These studies would provide physical and molecular insights into the processes that occur not only on the binding of the enzyme to the interface, but also those that occur on the binding of inhibitors and products to PLA2 at the interface. Specific mutants of PLA2 will also be used to identify the residues involved in the binding of the enzyme to the interface and the residues involved in the binding of ligands to the catalytic active site region.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of General Medical Sciences (NIGMS)
Type
Research Project (R01)
Project #
5R01GM029703-10
Application #
3277332
Study Section
Physical Biochemistry Study Section (PB)
Project Start
1983-04-01
Project End
1996-06-30
Budget Start
1993-07-01
Budget End
1994-06-30
Support Year
10
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
University of Delaware
Department
Type
Schools of Arts and Sciences
DUNS #
059007500
City
Newark
State
DE
Country
United States
Zip Code
19716

  Publications

Pan, Ying H; Bahnson, Brian J (2010) Structure of a premicellar complex of alkyl sulfates with the interfacial binding surfaces of four subunits of phospholipase A2. Biochim Biophys Acta 1804:1443-8
Pan, Ying H; Bahnson, Brian J (2007) Structural basis for bile salt inhibition of pancreatic phospholipase A2. J Mol Biol 369:439-50
Tsai, Yu-Cheng; Yu, Bao-Zhu; Wang, Yu-Zhen et al. (2006) Desolvation map of the i-face of phospholipase A2. Biochim Biophys Acta 1758:653-65
Bahnson, Brian J (2005) Structure, function and interfacial allosterism in phospholipase A2: insight from the anion-assisted dimer. Arch Biochem Biophys 433:96-106
Yu, Bao-Zhu; Polenova, Tatyana; Jain, Mahendra Kumar et al. (2005) Premicellar complexes of sphingomyelinase mediate enzyme exchange for the stationary phase turnover. Biochim Biophys Acta 1712:137-51
Yu, Bao-Zhu; Pan, Ying H; Janssen, Marcel J W et al. (2005) Kinetic and structural properties of disulfide engineered phospholipase A2: insight into the role of disulfide bonding patterns. Biochemistry 44:3369-79
Berg, Otto G; Yu, Bao-Zhu; Chang, Cherry et al. (2004) Cooperative binding of monodisperse anionic amphiphiles to the i-face: phospholipase A2-paradigm for interfacial binding. Biochemistry 43:7999-8013
Berg, Otto G; Yu, Bao-Zhu; Apitz-Castro, Rafael J et al. (2004) Phosphatidylinositol-specific phospholipase C forms different complexes with monodisperse and micellar phosphatidylcholine. Biochemistry 43:2080-90
Cajal, Yolanda; Berg, Otto G; Jain, Mahendra Kumar (2004) Origins of delays in monolayer kinetics: phospholipase A2 paradigm. Biochemistry 43:9256-64
Yu, Bao-Zhu; Apitz-Castro, Rafael; Tsai, Ming-Daw et al. (2003) Interaction of monodisperse anionic amphiphiles with the i-face of secreted phospholipase A2. Biochemistry 42:6293-301

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